- 作者:Rohit J. Lodhia ; rohitlodhi@gmail.com" class="auth_mail" title="E-mail the corresponding author ; Salaj Masandb ; Amna Malikc ; e ; Kuppuswami Shivakumard ; e ; Victoria D.M. McAllistere ; Veronica O'Keanef ; Leah C. Younga ; Adrian H. Healdg ; Roy A. Sherwoodh ; Katherine J. Aitchisona ; e ; i ; j
- 关键词:Bone markers ; Antipsychotics ; Ntxc ; Aripiprazole
- 刊名:Schizophrenia Research
- 出版年:2016
- 出版时间:February 2016
- 年:2016
- 卷:170
- 期:2-3
- 页码:245-251
- 全文大小:344 K
Method
A 52-week follow-up of patients switched to aripiprazole or with aripiprazole added on, conducting a specific analysis of markers of bone turnover: urinary NTX (a biomarker of bone resorption) and serum BSAP (a biomarker of bone formation). Baseline and serial measurements of bone markers NTX, BSAP and of hormones prolactin, oestrogen and testosterone were done at weeks 0 and 1, 2, 6, 12, 26 and 52, respectively.
Results
NTX concentration reduced over time but this did not reach significance in the whole group (log-NTX: β = − 0.0012, p = 0.142). For BSAP the addition of or replacement with aripiprazole produced a significant reduction (log-BSAP: β = − 0.00039, p = 0.002). Analysis with prolactin similarly showed a significant reduction (log-prolactin: β = − 0.0024, p < 0.001); other hormones did not change significantly. Sensitivity analysis to compare the switchers to aripiprazole versus the “add-on” showed that the former group had a significant reduction in NTX.
Conclusions
We found that switching to aripiprazole was associated with changes in molecular biomarkers of bone resorption, indicating a more favourable profile for bone health.